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NanoSIMS combined with fluorescence microscopy as a tool for subcellular imaging of isotopically labeled platinum-based anticancer drugs

机译:Nanosims与荧光显微镜相结合作为同位素标记的铂基抗癌药物亚细胞成像的工具

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Multi-elemental, isotope selective nano-scale secondary ion mass spectrometry (NanoSIMS) combined with confocal laser-scanning microscopy was used to characterize the subcellular distribution of ~(15) N-labeled cisplatin in human colon cancer cells. These analyses indicated predominant cisplatin colocalisation with sulfur-rich structures in both the nucleus and cytoplasm. Furthermore, colocalisation of platinum with phosphorus-rich chromatin regions was observed, which is consistent with its binding affinity to DNA as the generally accepted crucial target of the drug. Application of ~(15) N-labeled cisplatin and subsequent measurement of the nitrogen isotopic composition and determination of the relative intensities of platinum and nitrogen associated secondary ion signals in different cellular compartments with NanoSIMS suggested partial dissociation of Pt–N bonds during the accumulation process, in particular within nucleoli at elevated cisplatin concentrations. This finding raises the question as to whether the observed intracellular dissociation of the drug has implications for the mechanism of action of cisplatin. Within the cytoplasm, platinum mainly accumulated in acidic organelles, as demonstrated by a direct combination of specific fluorescent staining, confocal laser scanning microscopy and NanoSIMS. Different processing of platinum drugs in acidic organelles might be relevant for their detoxification, as well as for their mode of action.
机译:多元素的同位素选择性纳米级二次离子质谱(纳米粒子)与共聚焦激光扫描显微镜结合使用,表征了人结肠癌细胞中〜(15)标记顺铂的亚细胞分布。这些分析表明,在细胞核和细胞质中具有富含硫结构的主要顺铂层均匀化。此外,观察到具有富含磷染色质区的铂的分配,其与其对DNA的结合亲和力一致,因为通常所接受的药物的关键靶标。 〜(15)标记的顺铂及随后测量氮同位素组合物的施用和纳米粒子不同细胞室中铂和氮的相关二次离子信号的相对强度的测定表明在积累过程中PT-N键的部分解离PT-N键特别是在升高的顺铂浓度下的核仁内。这一发现提出了观察到药物的细胞内解离的问题对顺铂的作用机制有影响。在细胞质内,铂主要积聚在酸性细胞器中,如特定荧光染色,共聚焦激光扫描显微镜和纳米染料的直接组合所示。在酸性细胞器中的不同处理铂药物可能与其排毒以及它们的作用方式相关。

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